| Literature DB >> 28714964 |
J Rodriguez-Blanco1, L Pednekar1, C Penas2, B Li1, V Martin3, J Long1, E Lee4, W A Weiss5, C Rodriguez3, N Mehrdad6, D M Nguyen7,8, N G Ayad2,8, P Rai8,9, A J Capobianco1,8, D J Robbins1,8.
Abstract
The SMOOTHENED inhibitor vismodegib is FDA approved for advanced basal cell carcinoma (BCC), and shows promise in clinical trials for SONIC HEDGEHOG (SHH)-subgroup medulloblastoma (MB) patients. Clinical experience with BCC patients shows that continuous exposure to vismodegib is necessary to prevent tumor recurrence, suggesting the existence of a vismodegib-resistant reservoir of tumor-propagating cells. We isolated such tumor-propagating cells from a mouse model of SHH-subgroup MB and grew them as sphere cultures. These cultures were enriched for the MB progenitor marker SOX2 and formed tumors in vivo. Moreover, while their ability to self-renew was resistant to SHH inhibitors, as has been previously suggested, this self-renewal was instead WNT-dependent. We show here that loss of Trp53 activates canonical WNT signaling in these SOX2-enriched cultures. Importantly, a small molecule WNT inhibitor was able to reduce the propagation and growth of SHH-subgroup MB in vivo, in an on-target manner, leading to increased survival. Our results imply that the tumor-propagating cells driving the growth of bulk SHH-dependent MB are themselves WNT dependent. Further, our data suggest combination therapy with WNT and SHH inhibitors as a therapeutic strategy in patients with SHH-subgroup MB, in order to decrease the tumor recurrence commonly observed in patients treated with vismodegib.Entities:
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Year: 2017 PMID: 28714964 PMCID: PMC5680121 DOI: 10.1038/onc.2017.232
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867